Author:
Bangert Mathieu,Wright Adam K.,Rylance Jamie,Kelly Matthew J.,Wright Angela D.,Carlone George M.,Sampson Jacquelyn S.,Rajam Gowrisankar,Ades Edwin W.,Kadioglu Aras,Gordon Stephen B.
Abstract
ABSTRACTNew treatment strategies are urgently needed to overcome early mortality in acute bacterial infections. Previous studies have shown that administration of a novel immunoactivating peptide (P4) alongside passive immunotherapy prevents the onset of septicemia and rescues mice from lethal invasive disease models of pneumococcal pneumonia and sepsis. In this study, using two diverse populations of adult volunteers, we determined whether P4 treatment of human alveolar macrophages would upregulate phagocytic killing ofStreptococcus pneumoniaeex vivo. We also measured macrophage intracellular oxidation, cytokine secretion, and surface marker expression following stimulation. Peptide treatment showed enhanced bacterial killing in the absence of nonspecific inflammation, consistent with therapeutic potential. This is the first demonstration of P4 efficacy onex vivo-derived human lung cells.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
Cited by
8 articles.
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